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Discovery by Virtual Screening of an Inhibitor of CDK5-Mediated PPARγ Phosphorylation.

Gavin O'MahonyJens PetersenMargareta EkRebecca RaeCarina JohanssonLiu JianmingNina ProkophFredrik BergströmKrister BambergFabrizio GiordanettoBader ZarroukiDaniel KarlssonAnders Hogner
Published in: ACS medicinal chemistry letters (2022)
Thiazolidinedione PPARγ agonists such as rosiglitazone and pioglitazone are effective antidiabetic drugs, but side effects have limited their use. It has been posited that their positive antidiabetic effects are mainly mediated by the inhibition of the CDK5-mediated Ser273 phosphorylation of PPARγ, whereas the side effects are linked to classical PPARγ agonism. Thus compounds that inhibit PPARγ Ser273 phosphorylation but lack classical PPARγ agonism have been sought as safer antidiabetic therapies. Herein we report the discovery by virtual screening of 10 , which is a potent PPARγ binder and in vitro inhibitor of the CDK5-mediated phosphorylation of PPARγ Ser273 and displays negligible PPARγ agonism in a reporter gene assay. The pharmacokinetic properties of 10 are compatible with oral dosing, enabling preclinical in vivo testing, and a 7 day treatment demonstrated an improvement in insulin sensitivity in the ob/ob diabetic mouse model.
Keyphrases
  • insulin resistance
  • fatty acid
  • mouse model
  • high throughput
  • small molecule
  • type diabetes
  • adipose tissue
  • mesenchymal stem cells
  • cell proliferation
  • bone marrow
  • cell therapy